Modelling the Progression towards Duodenal Cancer among Patients with Familial Polyposis on the Basis of Two Different Score Profiles

The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specifi...

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Published in	European journal of epidemiology Vol. 20; no. 4; pp. 339 - 343
Main Authors	Gutknecht, C., Iwaz, J., Boutitie, F., Saurin, J.-C., Ecochard, R.
Format	Journal Article
Language	English
Published	Dordrecht Springer 01.04.2005 Springer Nature B.V Springer Verlag
Subjects	Adenoma Adenomatous polyposis coli Adenomatous Polyposis Coli - complications Adenomatous Polyposis Coli - physiopathology Adult Bayes Theorem Biological and medical sciences Cancer Cancer Epidemiology Disease models Disease Progression Duodenal Neoplasms - etiology Epidemiology Evolution Families & family life Female France Gastroenterology. Liver. Pancreas. Abdomen Gaussian distributions Heterogeneity Humans Intestinal neoplasms Life Sciences Linear Models Male Medical sciences Middle Aged Modeling Other Parametric models Patient assessment Population estimates Prognosis Prospective Studies Small intestine Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Tumors France Human Prognosis Duodenum Digestive system Familial adenomatous polyposis Mixture model Familial adenomatous polyposis coli Malignant tumor Small intestine Epidemiology Modeling Genetic disease Follow up study Duodenal cancer Digestive diseases Intestinal disease Evolution Models Public health Longitudinal model
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ISSN	0393-2990 1573-7284
DOI	10.1007/s10654-005-0371-x

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Abstract	The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups: stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35%. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score ≥9 is near 43% at age 60 (36-50%) and 50% at 70 (43-57%). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles.
AbstractList	The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score >/=9 is near 43% at age 60 (36-50) and 50 at 70 (43-57). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles.[PUBLICATION ABSTRACT] The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups: stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35%. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score > or = 9 is near 43% at age 60 (36-50%) and 50% at 70 (43-57%). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles. The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups: stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35%. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score > or = 9 is near 43% at age 60 (36-50%) and 50% at 70 (43-57%). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles.The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups: stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35%. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score > or = 9 is near 43% at age 60 (36-50%) and 50% at 70 (43-57%). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles. The objective was to design a method that considers, on clinical arguments, the likely existence of patient subgroups with different evolution profiles. The method is applied in familial adenomatous polyposis to predict the proportion of patients that would develop duodenal cancer. A subject-specific linear mixed-effects model was elaborated to explicitly model heterogeneity in regression parameters. The estimates of the parameters were obtained by Bayesian inference using Gibbs sampling. The application concerned two potential polyposis subgroups: stable-state and progressive. Each patient's score was expressed in function of his putative subgroup, the reference subgroup mean score (intercept), the rate of change (slope), and time. The estimated proportion of stable-state patients was 35%. In progressive-state patients, the estimated annual score increase was 0.38 (95% CI: 0.27-0.48). The regression model predicted that the proportion of patients with a score ≥9 is near 43% at age 60 (36-50%) and 50% at 70 (43-57%). The method indicates the evolution profile of each subject, which facilitates therapeutic decisions. The modelling may be extended to other more complex situations with several subgroups, with different change rates, or with various genetic or therapeutic profiles.
Author	Iwaz, J. Gutknecht, C. Ecochard, R. Saurin, J.-C. Boutitie, F.
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Keywords	Human Prognosis Duodenum Digestive system Familial adenomatous polyposis Mixture model Familial adenomatous polyposis coli Malignant tumor Small intestine Epidemiology Modeling Genetic disease Follow up study Duodenal cancer Digestive diseases Intestinal disease Evolution Models Public health Longitudinal model
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References	H Goldstein (CR7) 1995 M Lesperance (CR15) 2001 VT Farewell (CR1) 1982; 38 G Verbeke (CR6) 1996; 91 I Heiskanen (CR17) 1999; 31 GJ McLachlan (CR14) 1998 ML Arvanitis (CR12) 1990; 33 JC Saurin (CR8) 2004; 22 J Bjork (CR16) 2001; 121 KP Nugent (CR13) 1993; 36 CR11 AD Spigelman (CR9) 1989; 2 R Maller (CR2) 1996 WR Gilks (CR10) 1996 D Böhning (CR18) 1998; 54 LA Goodman (CR5) 1961; 56 P Maruani (CR3) 1983; 105 CR Weinberg (CR4) 1986; 42
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SubjectTerms	Adenoma Adenomatous polyposis coli Adenomatous Polyposis Coli - complications Adenomatous Polyposis Coli - physiopathology Adult Bayes Theorem Biological and medical sciences Cancer Cancer Epidemiology Disease models Disease Progression Duodenal Neoplasms - etiology Epidemiology Evolution Families & family life Female France Gastroenterology. Liver. Pancreas. Abdomen Gaussian distributions Heterogeneity Humans Intestinal neoplasms Life Sciences Linear Models Male Medical sciences Middle Aged Modeling Other Parametric models Patient assessment Population estimates Prognosis Prospective Studies Small intestine Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Tumors
Title	Modelling the Progression towards Duodenal Cancer among Patients with Familial Polyposis on the Basis of Two Different Score Profiles
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